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首页> 外文期刊>Chemical Engineering Research & Design: Transactions of the Institution of Chemical Engineers >Optimization of the formulation of solid multiparticulate dosage forms containing pancreatin
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Optimization of the formulation of solid multiparticulate dosage forms containing pancreatin

机译:含有胰酶的固体多颗粒剂型的配方优化

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The objective of this study was to investigate the changes in the starch-hydrolysing activity of pancreatin under conditions that can occur during the formulation of multiparticulate systems (granulation, direct compression for the preparation of minitablets and coating). Direct compression did not induce a significant alteration in the starch-hydrolysing activity. A factorial design was applied in the testing of the wet conditions ensured by water and ethanol. These had a significant impact, though ethanol caused a more relevant decrease. An increased content of liquid was necessary for unwanted effects, but the changes of its amount in the tested range were not highly relevant. In both cases, the most important factor in the investigation of wet conditions was temperature. During the study of the effects of modelling of the circumstances of tabletting, elevated temperature did not cause alterations in the relatively dry material. This information can promote an improved design for the preparation of the dosage form. Pelletization is not appropriate for the preparation of an intermediate. Direct compression is the most suitable formulation step. Coating must be performed at low temperature with aqueous systems, but rapid drying is also advisable for the first separating layer. A mathematically based optimization can be necessary for the preformulation study of the preparation of dosage forms containing sensitive enzymes.
机译:这项研究的目的是研究在配制多颗粒系统(制粒,直接压片以制备小片和包衣)过程中可能发生的条件下胰酶的淀粉水解活性的变化。直接压缩不引起淀粉水解活性的显着改变。析因设计应用于水和乙醇确保的潮湿条件的测试中。尽管乙醇引起了更相关的减少,但这些都产生了重大影响。增加液体含量对于产生不希望的效果是必要的,但是在测试范围内其量的变化并不是高度相关的。在这两种情况下,研究潮湿条件的最重要因素是温度。在研究压片情况的建模效果期间,升高温度不会引起相对干燥的材料发生变化。该信息可以促进用于剂型制备的改进设计。制粒不适用于中间体的制备。直接压缩是最合适的配制步骤。必须使用水性体系在低温下进行涂布,但是建议对第一隔离层进行快速干燥。对于包含敏感酶的剂型制剂的预配方研究,基于数学的优化可能是必需的。

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